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An Optimized Method for Delivering Flow Tracer Particles to Intravital Fluid Environments in the Developing Zebrafish

机译:在发育中的斑马鱼体内将流动示踪剂颗粒输送到体内流体环境的一种优化方法

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摘要

Growing evidence suggests that intravital flow–structure interactions are critical morphogens for normal embryonic development and disease progression, but fluid mechanical studies aimed at investigating these interactions have been limited in their ability to visualize and quantify fluid flow. In this study, we describe a protocol for injecting small (≤1.0 μm) tracer particles into fluid beds of the larval zebrafish to facilitate microscale fluid mechanical analyses. The microinjection apparatus and associated borosilicate pipette design, typically blunt-tipped with a 2–4 micron tip O.D., yielded highly linear (r2=0.99) in vitro bolus ejection volumes. The physical characteristics of the tracer particles were optimized for efficient particle delivery. Seeding densities suitable for quantitative blood flow mapping (≥50 thousand tracers per fish) were routinely achieved and had no adverse effects on zebrafish physiology or long-term survivorship. The data and methods reported here will prove valuable for a broad range of in vivo imaging technologies [e.g., particle-tracking velocimetry, μ-Doppler, digital particle image velocimetry (DPIV), and 4-dimensional-DPIV] which rely on tracer particles to visualize and quantify fluid flow in the developing zebrafish.
机译:越来越多的证据表明,活体内流与结构的相互作用是正常胚胎发育和疾病进展的关键形态发生子,但是旨在研究这些相互作用的流体力学研究在可视化和量化流体流动的能力方面受到限制。在这项研究中,我们描述了将小(≤1.0μm)示踪剂粒子注入幼虫斑马鱼的流化床中以促进微观流体力学分析的方案。显微注射装置和相关的硼硅酸盐移液器设计通常使用2到4微米尖端外径进行钝头处理,可产生高度线性(r 2 = 0.99)的体外大剂量推注体积。优化了示踪剂颗粒的物理特性,以实现有效的颗粒输送。常规地获得了适合定量血流分布图的播种密度(每条鱼≥5万个示踪物),并且对斑马鱼的生理或长期生存没有不利影响。此处报道的数据和方法将证明对依赖示踪剂颗粒的多种体内成像技术(例如,颗粒跟踪测速,μ-多普勒,数字颗粒图像测速(DPIV)和4维-DPIV)有价值。可视化和量化正在发育的斑马鱼中的流体流动。

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